Effectiveness of Metyrapone in Treating Cushing's Syndrome: A Retrospective Multicenter Study in 195 Patients

Eleni Daniel; Simon Aylwin; Omar Mustafa; Steve Ball; Atif Munir; Kristien Boelaert; Vasileios Chortis; Daniel J Cuthbertson; Christina Daousi; Surya P Rajeev; Julian Davis; Kelly Cheer; William Drake; Kirun Gunganah; Ashley Grossman; Mark Gurnell; Andrew S Powlson; Niki Karavitaki; Isabel Huguet; Tara Kearney; Kumar Mohit; Karim Meeran; Neil Hill; Aled Rees; Andrew J Lansdown; Peter J Trainer; Anna-Elisabeth H Minder; John Newell-Price

doi:10.1210/jc.2015-2616

Effectiveness of Metyrapone in Treating Cushing's Syndrome: A Retrospective Multicenter Study in 195 Patients

J Clin Endocrinol Metab. 2015 Nov;100(11):4146-54. doi: 10.1210/jc.2015-2616. Epub 2015 Sep 9.

Authors

Eleni Daniel¹, Simon Aylwin¹, Omar Mustafa¹, Steve Ball¹, Atif Munir¹, Kristien Boelaert¹, Vasileios Chortis¹, Daniel J Cuthbertson¹, Christina Daousi¹, Surya P Rajeev¹, Julian Davis¹, Kelly Cheer¹, William Drake¹, Kirun Gunganah¹, Ashley Grossman¹, Mark Gurnell¹, Andrew S Powlson¹, Niki Karavitaki¹, Isabel Huguet¹, Tara Kearney¹, Kumar Mohit¹, Karim Meeran¹, Neil Hill¹, Aled Rees¹, Andrew J Lansdown¹, Peter J Trainer¹, Anna-Elisabeth H Minder¹, John Newell-Price¹

Affiliation

¹ The Medical School (E.D., J.N.-P.), University of Sheffield, S10 2RX Sheffield, United Kingdom; King's College Hospital NHS Foundation Trust (S.A., O.M.), B15 2TT London, United Kingdom; The Medical School (S.B.), Newcastle University, NE2 4HH Newcastle, United Kingdom; Royal Victoria Infirmary (S.B., A.M.), SE5 9RS Newcastle, United Kingdom; College of Medical and Dental Sciences (K.B., V.C., N.K.), Centre for Endocrinology, Diabetes and Metabolism, University of Birmingham, M13 9PT Birmingham, United Kingdom; Department of Obesity and Endocrinology (D.J.C., C.D., S.P.R.), University of Liverpool, NE1 4LP Liverpool, United Kingdom; Centre for Endocrinology and Diabetes (J.D.), University of Manchester, L69 3GA Manchester, United Kingdom; Manchester Royal Infirmary (K.C.), M13 9WL Manchester, United Kingdom; Department of Endocrinology (W.D., K.G.), St Bartholomew's Hospital, EC1A 7BE London, United Kingdom; Oxford Centre for Diabetes (A.G., N.K., I.H.), Endocrinology and Metabolism, Churchill Hospital, M6 8HD Oxford, United Kingdom; Wellcome Trust-MRC Institute of Metabolic Science (M.G., A.S.P.), University of Cambridge, Addenbrooke's Hospital, OX3 7LE Cambridge, United Kingdom; Salford Royal Foundation Trust (T.K., K.Mo.), CB2 0QQ Salford, United Kingdom; Imperial College (K.Me., N.H.), SW7 2AZ London, United Kingdom; School of Medicine (A.R., A.J.L.), Cardiff University, CF14 4XN Cardiff, United Kingdom; and The Christie NHS Foundation Trust (P.J.T., A.-E.H.M.), M20 4BX Manchester, United Kingdom.

Abstract

Background: Cushing's syndrome (CS) is a severe condition with excess mortality and significant morbidity necessitating control of hypercortisolemia. There are few data documenting use of the steroidogenesis inhibitor metyrapone for this purpose.

Objective: The objective was to assess the effectiveness of metyrapone in controlling cortisol excess in a contemporary series of patients with CS.

Design: This was designed as a retrospective, multicenter study.

Setting: Thirteen University hospitals were studied.

Patients: We studied a total of 195 patients with proven CS: 115 Cushing's disease, 37 ectopic ACTH syndrome, 43 ACTH-independent disease (adrenocortical carcinoma 10, adrenal adenoma 30, and ACTH-independent adrenal hyperplasia 3).

Measurements: Measurements included biochemical parameters of activity of CS: mean serum cortisol "day-curve" (CDC) (target 150-300 nmol/L); 9 am serum cortisol; 24-hour urinary free cortisol (UFC).

Results: A total of 164/195 received metyrapone monotherapy. Mean age was 49.6 ± 15.7 years; mean duration of therapy 8 months (median 3 mo, range 3 d to 11.6 y). There were significant improvements on metyrapone, first evaluation to last review: CDC (91 patients, 722.9 nmol/L [26.2 μg/dL] vs 348.6 nmol/L [12.6 μg/dL]; P < .0001); 9 am cortisol (123 patients, 882.9 nmol/L [32.0 μg/dL] vs 491.1 nmol/L [17.8 μg/dL]; P < .0001); and UFC (37 patients, 1483 nmol/24 h [537 μg/24 h] vs 452.6 nmol/24 h [164 μg/24 h]; P = .003). Overall, control at last review: 55%, 43%, 46%, and 76% of patients who had CDCs, UFCs, 9 am cortisol less than 331 nmol/L (12.0 μg/dL), and 9 am cortisol less than upper limit of normal/600 nmol/L (21.7 μg/dL). Median final dose: Cushing's disease 1375 mg; ectopic ACTH syndrome 1500 mg; benign adrenal disease 750 mg; and adrenocortical carcinoma 1250 mg. Adverse events occurred in 25% of patients, mostly mild gastrointestinal upset and dizziness, usually within 2 weeks of initiation or dose increase, all reversible.

Conclusions: Metyrapone is effective therapy for short- and long-term control of hypercortisolemia in CS.

Publication types

Multicenter Study
Research Support, Non-U.S. Gov't

MeSH terms

ACTH-Secreting Pituitary Adenoma / drug therapy
Adolescent
Adult
Aged
Aged, 80 and over
Child
Child, Preschool
Cushing Syndrome / drug therapy*
Dose-Response Relationship, Drug
Drug Therapy, Combination
Enzyme Inhibitors / administration & dosage
Enzyme Inhibitors / adverse effects
Enzyme Inhibitors / therapeutic use*
Humans
Hydrocortisone / blood
Hydrocortisone / urine
Infant
Male
Metyrapone / administration & dosage
Metyrapone / adverse effects
Metyrapone / therapeutic use*
Middle Aged
Pituitary Neoplasms / drug therapy
Retrospective Studies
Treatment Outcome
Young Adult

Substances

Enzyme Inhibitors
Hydrocortisone
Metyrapone